Literature DB >> 16909111

FMIP controls the adipocyte lineage commitment of C2C12 cells by downmodulation of C/EBP alpha.

A Mancini1, O El Bounkari, A-F Norrenbrock, M Scherr, D Schaefer, M Eder, A H Banham, K Pulford, L Lyne, A D Whetton, T Tamura.   

Abstract

Fms interacting protein (FMIP) is a substrate for Fms tyrosine kinase, and a nuclear/cytoplasm shuttling protein with a leucine zipper. As the phosphorylation of FMIP is observed in insulin-stimulated preadipocytes, we examined the role of FMIP in adipocyte differentiation, using the mesenchymal multipotent stem cells, C2C12 cells, that can differentiate into adipocytes, muscle cells and osteoblasts. Ectopic expression of FMIP in C2C12 impairs the adipocyte differentiation induced by treatment with insulin, dexamethasone and 3-isobutyl-1-methylxanthine. These cells exhibit muscle phenotype with multinuclear morphology. Furthermore, knockdown of endogenous FMIP expression by small interfering RNA improves adipocytic lineage commitment of C2C12 cells, while impairing muscle differentiation. Upon stimulation with insulin, CCAAT/enhancer binding protein (C/EBP)beta, but not C/EBPalpha, is upregulated in cells expressing ectopic FMIP, whereas in FMIP knockdown cells, C/EBPalpha is constitutively expressed. Ectopic expression of C/EBPalpha counteracts the effects of FMIP, whereas C/EBPalpha knockdown partially mimics the effects of FMIP in this system. Northern blot analysis and reverse transcriptase-polymerase chain reaction study reveal that ectopic FMIP-expressing cells do not contain the polyadenylated C/EBPalpha mRNA, but contain the C/EBPalpha pre-mRNA, suggesting that FMIP plays a role in RNA processing and/or export. Indeed, a member of the THO complex that plays a role in mRNA export, THOC1, is co-precipitated with FMIP. The data we have acquired on FMIP suggest that it is a target for tyrosine kinase receptors that potentiate mRNA export.

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Year:  2006        PMID: 16909111     DOI: 10.1038/sj.onc.1209853

Source DB:  PubMed          Journal:  Oncogene        ISSN: 0950-9232            Impact factor:   9.867


  20 in total

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2.  Pax3 induces differentiation of juvenile skeletal muscle stem cells without transcriptional upregulation of canonical myogenic regulatory factors.

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3.  THOC5: a novel gene involved in HDL-cholesterol metabolism.

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Journal:  J Lipid Res       Date:  2013-09-10       Impact factor: 5.922

4.  C/EBPβ mediates tumour-induced ubiquitin ligase atrogin1/MAFbx upregulation and muscle wasting.

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Journal:  EMBO J       Date:  2011-08-16       Impact factor: 11.598

5.  Identification of mRNAs that are spliced but not exported to the cytoplasm in the absence of THOC5 in mouse embryo fibroblasts.

Authors:  Anuja Guria; Doan Duy Hai Tran; Sheetal Ramachandran; Alexandra Koch; Omar El Bounkari; Priyanka Dutta; Hansjörg Hauser; Teruko Tamura
Journal:  RNA       Date:  2011-04-27       Impact factor: 4.942

6.  Oxidative stress-induced S100B accumulation converts myoblasts into brown adipocytes via an NF-κB/YY1/miR-133 axis and NF-κB/YY1/BMP-7 axis.

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7.  Signaling mechanism of tumor cell-induced up-regulation of E3 ubiquitin ligase UBR2.

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Review 9.  Messenger RNA export from the nucleus: a series of molecular wardrobe changes.

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Journal:  Traffic       Date:  2009-06-27       Impact factor: 6.215

10.  THOC5/FMIP, an mRNA export TREX complex protein, is essential for hematopoietic primitive cell survival in vivo.

Authors:  Annalisa Mancini; Susanne C Niemann-Seyde; Rüdiger Pankow; Omar El Bounkari; Sabine Klebba-Färber; Alexandra Koch; Ewa Jaworska; Elaine Spooncer; Achim D Gruber; Anthony D Whetton; Teruko Tamura
Journal:  BMC Biol       Date:  2010-01-05       Impact factor: 7.431

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